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Article ? AI-assigned paper type based on the abstract. Classification may not be perfect — flag errors using the feedback button. Tier 2 ? Original research — experimental, observational, or case-control study. Direct primary evidence. Human Health Effects Nanoplastics Sign in to save

Maternal exposure to polystyrene nanoplastics causes defective retinal development and function in progeny mice by disturbing metabolic profiles

Chemosphere 2024 30 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 65 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Guangquan Chen, Guangquan Chen, Jincan He, Shiyi Xiong, Hao Qiu, Shiyi Xiong, Cornelis A.M. van Gestel Guangquan Chen, Guangquan Chen, Guangquan Chen, Erkai He, Shiyi Xiong, Erkai He, Hao Qiu, Hao Qiu, Hao Qiu, Hao Qiu, Erkai He, Erkai He, Erkai He, Erkai He, Shiyi Xiong, Erkai He, Cornelis A.M. van Gestel Jincan He, Jing Li, Jing Li, Jing Li, Jing Li, Jing Li, Shiyi Xiong, Cornelis A.M. van Gestel Guangquan Chen, Guangquan Chen, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Erkai He, Erkai He, Erkai He, Erkai He, Erkai He, Cornelis A.M. van Gestel Jing Li, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Shiyi Xiong, Cornelis A.M. van Gestel Hao Qiu, Erkai He, Hao Qiu, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Erkai He, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Jing Li, Liang Cao, Hao Qiu, Hao Qiu, Guangquan Chen, Cornelis A.M. van Gestel Erkai He, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Erkai He, Cornelis A.M. van Gestel Erkai He, Hao Qiu, Hao Qiu, Hao Qiu, Hao Qiu, Jing Li, Jing Li, Jing Li, Jing Li, Jing Li, Jing Li, Erkai He, Cornelis A.M. van Gestel Jing Li, Hao Qiu, Hao Qiu, Hao Qiu, Hao Qiu, Zhengdong Qiao, Hao Qiu, Hao Qiu, Zhengdong Qiao, Hao Qiu, Erkai He, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Erkai He, Hao Qiu, Hao Qiu, Hao Qiu, Liang Cao, Liang Cao, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Jing Li, Jing Li, Jing Li, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Hao Qiu, Cornelis A.M. van Gestel Hao Qiu, Hao Qiu, Jing Li, Hao Qiu, Hao Qiu, Hao Qiu, Jing Li, Hao Qiu, Guangquan Chen, Guangquan Chen, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Shiyi Xiong, Hao Qiu, Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel Cornelis A.M. van Gestel

Summary

When pregnant mice drank water containing nanoplastics at levels found in the environment, their pups were born with defective eye development -- fewer retinal nerve cells, slower blood vessel growth in the retina, and abnormal visual function. The nanoplastics disrupted key amino acids needed for normal retinal development. This is one of the first studies to show that prenatal nanoplastic exposure can harm eye development in offspring.

Polymers
Models
Study Type Environmental

Microplastics (MPs) and nanoplastics (NPs) are widely spreading in our living environment, accumulating in the human body and potentially threating human health. The retina, which is a terminally differentiated extension of the central nervous system, is essential for the visual system. However, the effects and molecular mechanisms of MPs/NPs on retina development and function are still unclear. Here, we investigated the effects and modes of action of polystyrene NPs (PS-NPs) on the retina using mice as a mammalian model species. Maternal PS-NP exposure (100 nm) at an environmentally realistic concentration of 10 mg L (or 2.07 *10 particles mL) via drinking water from the first day of pregnancy till the end of lactation (21 days after birth) caused defective neural retinal development in the neonatal mice, by depositing in the retinal tissue and reducing the number of retinal ganglion cells and bipolar cells. Exposure to PS-NPs retarded retinal vascular development, while abnormal electroretinogram (ERG) responses and an increased level of oxidative stress were also observed in the retina of the progeny mice after maternal PS-NP exposure. Metabolomics showed significant dysregulation of amino acids that are pivotal to neuron retinal function, such as glutamate, aspartate, alanine, glycine, serine, threonine, taurine, and serotonin. Transcriptomics identified significantly dysregulated genes, which were enriched in processes of angiogenesis, visual system development and lens development. Regulatory analysis showed that Fos gene mediated pathways could be a potential key target for PS-NP exposure in retinal development and function. Our study revealed that maternal exposure to PS-NPs generated detrimental effects on retinal development and function in progeny mice, offering new insights into the visual toxicity of PS-NPs.

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